Sensitive Testing of Plasma HIV-1 RNA and Sanger Sequencing of Cellular HIV-1 DNA for the Detection of Drug Resistance Prior to Starting First-line Antiretroviral Therapy with Etravirine or Efavirenz

Overview

Journal J Antimicrob Chemother

Publisher Oxford University Press

Specialty Infectious Diseases

Date 2013 Nov 29

PMID 24284781

Citations 12

Authors

Anna Maria Geretti

Tim Conibear

Andrew Hill

Jeffrey A Johnson

Lotke Tambuyzer

Kim Thys

Johan Vingerhoets

Yvon van Delft

Affiliations

Soon will be listed here.

Abstract

Objectives: This study investigated strategies that may increase the yield of drug resistance testing prior to starting antiretroviral therapy (ART), and whether transmitted and polymorphic resistance-associated mutations (RAMs) correlated with virological outcomes.

Methods: We carried out retrospective testing of baseline samples from patients entering the SENSE trial of first-line ART in Europe, Russia and Israel. Prior to randomization to etravirine or efavirenz plus two nucleos(t)ide reverse transcriptase inhibitors (NRTIs), plasma samples underwent routine Sanger sequencing of HIV-1 RT and protease ((plasma)SS) in order to exclude patients with transmitted RAMs. Retrospectively, Sanger sequencing was repeated with HIV-1 DNA from baseline peripheral blood mononuclear cells (PBMCSS); baseline plasma samples were retested by allele-specific PCR targeting seven RT RAMs (AS-PCR) and ultra-deep RT sequencing (UDS).

Results: By (plasma)SS, 16/193 (8.3%) patients showed ≥ 1 transmitted RAM affecting the NRTIs (10/193, 5.2%), non-nucleoside reverse transcriptase inhibitors (4/193, 2.1%) or protease inhibitors (2/193, 1.0%). No additional RAMs were detected by AS-PCR (n = 152) and UDS (n = 24); PBMCSS (n = 91) yielded two additional samples with one RAM each. Over 48 weeks, 4/79 (5.1%) patients on etravirine and 7/78 (9.0%) on efavirenz experienced virological failure; none had baseline RAMs. Conversely, 11/79 (13.9%) patients randomized to etravirine had one polymorphic RAM from the etravirine score in baseline plasma (V90I, V106I or E138A), without any impact on virological outcomes.

Conclusions: The detection of resistance increased marginally with PBMC testing but did not increase with sensitive plasma testing. A careful consideration is required of the cost-effectiveness of different strategies for baseline HIV drug resistance testing.

Citing Articles

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Abdullahi A, Diaz A, Fopoussi O, Beloukas A, Fokom Defo V, Kouanfack C J Antimicrob Chemother. 2023; 79(2):339-348.

PMID: 38153241 PMC: 10832591. DOI: 10.1093/jac/dkad386.

Optimizing Antiretroviral Therapy in Heavily ART-Experienced Patients with Multi-Class Resistant HIV-1 Using Proviral DNA Genotypic Resistance Testing.

Rauschning D, Ehren I, Heger E, Knops E, Fatkenheuer G, Suarez I Viruses. 2023; 15(7).

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HIV-1 DNA Testing in Viremic Patients Identifies More Drug Resistance Than HIV-1 RNA Testing.

Curanovic D, Martens S, Rodriguez M, Hammill H, Petropoulos C, Walworth C Open Forum Infect Dis. 2023; 10(4):ofad146.

PMID: 37065991 PMC: 10096913. DOI: 10.1093/ofid/ofad146.

HIV DNA Sequencing to Detect Archived Antiretroviral Drug Resistance.

Geretti A, Blanco J, Marcelin A, Perno C, Stellbrink H, Turner D Infect Dis Ther. 2022; 11(5):1793-1803.

PMID: 35915392 PMC: 9617980. DOI: 10.1007/s40121-022-00676-y.

Pre-existing singleton E138A mutations in the reverse transcriptase gene do not affect the efficacy of first-line antiretroviral therapy regimens using rilpivirine in human immunodeficiency virus-infected patients.

Kuznetsova A, Lebedev A, Gromov K, Kazennova E, Zazzi M, Incardona F Clin Case Rep. 2022; 10(2):e05373.

PMID: 35140966 PMC: 8813671. DOI: 10.1002/ccr3.5373.